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γ干扰素、白细胞介素2以及一种不同于γ干扰素和白细胞介素2的第三种因子在人B细胞增殖中的作用分析。有证据表明它们在B细胞活化后的不同时间发挥作用。

Analysis of the role of interferon-gamma, interleukin 2 and a third factor distinct from interferon-gamma and interleukin 2 in human B cell proliferation. Evidence that they act at different times after B cell activation.

作者信息

Romagnani S, Giudizi G M, Almerigogna F, Biagiotti R, Alessi A, Mingari C, Liang C M, Moretta L, Ricci M

出版信息

Eur J Immunol. 1986 Jun;16(6):623-9. doi: 10.1002/eji.1830160607.

Abstract

Recombinant interferon-gamma (rIFN-gamma) was able to induce proliferation of human tonsillar B cells activated with suboptimal concentrations of anti-mu antibody. The B cell growth factor (BCGF) activity of rIFN-gamma was not due to substances contaminating the IFN-gamma preparation, nor was it mediated by factors released by T cells or large granular lymphocytes following activation by rIFN-gamma. The response of B cells to rIFN-gamma peaked on day 3 of culture and rapidly declined thereafter, whereas the response of parallel anti-mu-activated B cell cultures to recombinant interleukin 2 (rIL2) appeared on day 3, but continued at least until day 5. In addition, B cells responsive to rIFN-gamma could be at least in part separated from those responsive to rIL2, the former being primarily contained in B cell fractions enriched for high-density small B lymphocytes. Finally, the addition to anti-mu-stimulated B cell cultures of very low concentrations of rIFN-gamma potentiated the B cell proliferation promoted by rIL2. The simultaneous addition of monoclonal antibodies against IFN-gamma and T cell activation antigen to anti-mu-stimulated B cell cultures strongly reduced the B cell proliferative response promoted by three different crude BCGF preparations obtained by polyclonal T cell activation in mixed lymphocyte culture. However, the supernatant from a T cell clone (DP5/11) apparently free of IL2, which manifested a BCGF activity similar to that of rIFN-gamma, still maintained its ability to promote proliferation of anti-mu-activated B cells after complete removal of IFN-gamma. Taken together, our data indicate that although some T cell clones are able to produce a BCGF distinct from both IFN-gamma and IL2, these lymphokines account for most of the BCGF activity of supernatants obtained from polyclonal T cell populations. They also suggest that IFN-gamma and the BCGF distinct from IFN-gamma and IL2 act primarily in the earlier phases of B cell activation and potentiate the proliferative response of activated B cells to IL2.

摘要

重组干扰素-γ(rIFN-γ)能够诱导被次优浓度抗μ抗体激活的人扁桃体B细胞增殖。rIFN-γ的B细胞生长因子(BCGF)活性并非源于污染IFN-γ制剂的物质,也不是由rIFN-γ激活后的T细胞或大颗粒淋巴细胞释放的因子介导的。B细胞对rIFN-γ的反应在培养第3天达到峰值,此后迅速下降,而平行的抗μ激活B细胞培养物对重组白细胞介素2(rIL2)的反应在第3天出现,但至少持续到第5天。此外,对rIFN-γ有反应的B细胞至少部分可与对rIL2有反应的B细胞分离,前者主要存在于富含高密度小B淋巴细胞的B细胞组分中。最后,向抗μ刺激的B细胞培养物中添加极低浓度的rIFN-γ可增强rIL2促进的B细胞增殖。将抗IFN-γ和T细胞激活抗原的单克隆抗体同时添加到抗μ刺激的B细胞培养物中,可强烈降低由混合淋巴细胞培养中多克隆T细胞激活获得的三种不同粗制BCGF制剂促进的B细胞增殖反应。然而,来自一个显然不含IL2的T细胞克隆(DP5/11)的上清液,其表现出与rIFN-γ相似的BCGF活性,在完全去除IFN-γ后仍保持促进抗μ激活B细胞增殖的能力。综上所述,我们的数据表明,尽管一些T细胞克隆能够产生一种不同于IFN-γ和IL2的BCGF,但这些淋巴因子占多克隆T细胞群体获得的上清液中大部分BCGF活性。它们还表明,IFN-γ以及不同于IFN-γ和IL2的BCGF主要在B细胞激活的早期阶段起作用,并增强激活的B细胞对IL2的增殖反应。

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